Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model

Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model

A model of pulmonary cryptococcosis in immunocompetent rats was developed to better understand the virulence of Cryptococcus gattii. Six isolates were studied, representing four molecular genotypes (VGI-MATα, VGIIa-MATα, VGIIa-MATa, VGIIb-MATα), obtained from Australia, Vancouver (Canada) and Colomb...

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Main Authors: Mark B. Krockenberger, Richard Malik, Popchai Ngamskulrungroj, Luciana Trilles, Patricia Escandon, Susan Dowd, Chris Allen, Uwe Himmelreich, Paul J. Canfield, Tania C. Sorrell, Wieland Meyer
Other Authors: The University of Sydney
Format: Article
Published: 2018
Subjects:
Agricultural and Biological Sciences
Immunology and Microbiology
Online Access:https://repository.li.mahidol.ac.th/handle/123456789/28442
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spelling th-mahidol.284422018-09-24T16:03:59Z Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model Mark B. Krockenberger Richard Malik Popchai Ngamskulrungroj Luciana Trilles Patricia Escandon Susan Dowd Chris Allen Uwe Himmelreich Paul J. Canfield Tania C. Sorrell Wieland Meyer The University of Sydney Mahidol University Fundacao Oswaldo Cruz Instituto Nacional de Salud Max Planck Institute for Metabolism Research Royal Children's Hospital Brisbane Agricultural and Biological Sciences Immunology and Microbiology A model of pulmonary cryptococcosis in immunocompetent rats was developed to better understand the virulence of Cryptococcus gattii. Six isolates were studied, representing four molecular genotypes (VGI-MATα, VGIIa-MATα, VGIIa-MATa, VGIIb-MATα), obtained from Australia, Vancouver (Canada) and Colombia. These originated from human patients, a cat and the environment and were administered intratracheally (i.t.) or transthoracically into Fischer 344 or Wistar-Furth rats in doses varying from 104to 107colony-forming units (CFU) in 0.1 ml of saline. With the exception of animals given the VGIIa-MATa isolate, rats consistently became ill or died of progressive cryptococcal pneumonia following i.t. doses exceeding 107CFU. Affected lungs increased in weight up to tenfold and contained numerous circumscribed, gelatinous lesions. These became larger and more extensive, progressing from limited hilar and/or tracheal lesions, to virtually confluent gelatinous masses. Disease was localized to the lungs for at least 3-4 weeks, with dissemination to the brain occurring in some animals after day 29. The dose-response relationship was steep for two VGI isolates studied (human WM179, environmental WM276); doses up to 106CFU i.t. did not produce lesions, while 107or more yeast cells produced progressive pneumonia. Intratracheal inoculation of rats with C. gattii provides an excellent model of human pulmonary cryptococcosis in healthy hosts, mimicking natural infections. Disease produced by C. gattii in rats is distinct from that caused by C. neoformans in that infections are progressive and ultimately fatal. © 2010 Springer Science+Business Media B.V. 2018-09-24T08:37:12Z 2018-09-24T08:37:12Z 2010-11-01 Article Mycopathologia. Vol.170, No.5 (2010), 315-330 10.1007/s11046-010-9328-z 0301486X 2-s2.0-78049337475 https://repository.li.mahidol.ac.th/handle/123456789/28442 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=78049337475&origin=inward
institution Mahidol University
building Mahidol University Library
continent Asia
country Thailand
Thailand
content_provider Mahidol University Library
collection Mahidol University Institutional Repository
topic Agricultural and Biological Sciences
Immunology and Microbiology
spellingShingle Agricultural and Biological Sciences
Immunology and Microbiology
Mark B. Krockenberger
Richard Malik
Popchai Ngamskulrungroj
Luciana Trilles
Patricia Escandon
Susan Dowd
Chris Allen
Uwe Himmelreich
Paul J. Canfield
Tania C. Sorrell
Wieland Meyer
Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
description A model of pulmonary cryptococcosis in immunocompetent rats was developed to better understand the virulence of Cryptococcus gattii. Six isolates were studied, representing four molecular genotypes (VGI-MATα, VGIIa-MATα, VGIIa-MATa, VGIIb-MATα), obtained from Australia, Vancouver (Canada) and Colombia. These originated from human patients, a cat and the environment and were administered intratracheally (i.t.) or transthoracically into Fischer 344 or Wistar-Furth rats in doses varying from 104to 107colony-forming units (CFU) in 0.1 ml of saline. With the exception of animals given the VGIIa-MATa isolate, rats consistently became ill or died of progressive cryptococcal pneumonia following i.t. doses exceeding 107CFU. Affected lungs increased in weight up to tenfold and contained numerous circumscribed, gelatinous lesions. These became larger and more extensive, progressing from limited hilar and/or tracheal lesions, to virtually confluent gelatinous masses. Disease was localized to the lungs for at least 3-4 weeks, with dissemination to the brain occurring in some animals after day 29. The dose-response relationship was steep for two VGI isolates studied (human WM179, environmental WM276); doses up to 106CFU i.t. did not produce lesions, while 107or more yeast cells produced progressive pneumonia. Intratracheal inoculation of rats with C. gattii provides an excellent model of human pulmonary cryptococcosis in healthy hosts, mimicking natural infections. Disease produced by C. gattii in rats is distinct from that caused by C. neoformans in that infections are progressive and ultimately fatal. © 2010 Springer Science+Business Media B.V.
author2 The University of Sydney
author_facet The University of Sydney
Mark B. Krockenberger
Richard Malik
Popchai Ngamskulrungroj
Luciana Trilles
Patricia Escandon
Susan Dowd
Chris Allen
Uwe Himmelreich
Paul J. Canfield
Tania C. Sorrell
Wieland Meyer
format Article
author Mark B. Krockenberger
Richard Malik
Popchai Ngamskulrungroj
Luciana Trilles
Patricia Escandon
Susan Dowd
Chris Allen
Uwe Himmelreich
Paul J. Canfield
Tania C. Sorrell
Wieland Meyer
author_sort Mark B. Krockenberger
title Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
title_short Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
title_full Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
title_fullStr Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
title_full_unstemmed Pathogenesis of pulmonary Cryptococcus gattii infection: A rat model
title_sort pathogenesis of pulmonary cryptococcus gattii infection: a rat model
publishDate 2018
url https://repository.li.mahidol.ac.th/handle/123456789/28442
_version_ 1763497723331346432

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